Diastereomerization process

Industrial Synthetic Improvements. One significant modification of the Stembach process is the result of work by Sumitomo chemists in 1975, in which the optical resolution—reduction sequence is replaced with a more efficient asymmetric conversion of the meso-cyc. 02Lcid (13) to the optically pure i7-lactone (17) (Fig. 3) (25). The cycloacid is reacted with the optically active dihydroxyamine [2964-48-9] (23) to quantitatively yield the chiral imide [85317-83-5] (24). Diastereoselective reduction of the pro-R-carbonyl using sodium borohydride affords the optically pure hydroxyamide [85317-84-6] (25) after recrystaUization. Acid hydrolysis of the amide then yields the desired i7-lactone (17). A similar approach uses chiral alcohols to form diastereomic half-esters stereoselectivity. These are reduced and direedy converted to i7-lactone (26). In both approaches, the desired diastereomeric half-amide or half-ester is formed in excess, thus avoiding the cosdy resolution step required in the Stembach synthesis. 

Although there is usually a preference for anti elimination in acyclic systems, syn elimination is competitive in some cases. In acyclic systems, the extent of anti versus syn elimination can be determined by use of stereospecifically deuterated substrates or by use of diastereomeric reactants which will give different products by syn and anti elimination. The latter approach showed that elimination from 3-phenyl-2-butyl tosylate is a stereospecific anti process. ... 

In recent years, several modifications of the Darzens condensation have been reported. Similar to the aldol reaction, the majority of the work reported has been directed toward diastereo- and enantioselective processes. In fact, when the aldol reaction is highly stereoselective, or when the aldol product can be isolated, useful quantities of the required glycidic ester can be obtained. Recent reports have demonstrated that diastereomeric enolate components can provide stereoselectivity in the reaction examples include the camphor-derived substrate 26, in situ generated a-bromo-A -... 

At present moment, no generally feasible method exists for the large-scale production of optically pure products. Although for the separation of virtually every racemic mixture an analytical method is available (gas chromatography, liquid chromatography or capillary electrophoresis), this is not the case for the separation of racemic mixtures on an industrial scale. The most widely applied method for the separation of racemic mixtures is diastereomeric salt crystallization [1]. However, this usually requires many steps, making the process complicated and inducing considerable losses of valuable product. In order to avoid the problems associated with diastereomeric salt crystallization, membrane-based processes may be considered as a viable alternative. 

As a unichiral group which reacts with the racemate to form diastereomeric molecules which can be separated by achiral adsorption processes. 

Scheme 5 details the asymmetric synthesis of dimethylhydrazone 14. The synthesis of this fragment commences with an Evans asymmetric aldol condensation between the boron enolate derived from 21 and trans-2-pentenal (20). Syn aldol adduct 29 is obtained in diastereomerically pure form through a process which defines both the relative and absolute stereochemistry of the newly generated stereogenic centers at carbons 29 and 30 (92 % yield). After reductive removal of the chiral auxiliary, selective silylation of the primary alcohol furnishes 30 in 71 % overall yield. The method employed to achieve the reduction of the C-28 carbonyl is interesting and worthy of comment. The reaction between tri-n-butylbor-... 

As well as the addition of achiral organometallic reagents to chiral aldehydes (see also Sections 1.3.2. and 1.3.3.), the addition of chiral organometallic reagents to carbonyl compounds is a well-known and intensively studied process which may lead to enantiomerically and/or diastereomerically enriched products. Chiral organometallic reagents can be classified into three groups ... 

Racemic l-methyl-2-butenylboronates (E)- and (Z)-3 may be prepared selectively via reactions of the l-methyl-2-butenyl Grignard reagent with the appropriate borate ester. Use of triisopropyl borate provides a 96 4 mixture of (E)-3l(Z)-3 on a 0.36 mol scale15. Use of a bulkier borylating agent, such as 2-isopropyloxy-4,4,5,5-tetramethyl-l,3,2-dioxaborolane, reverses the selectivity, enabling a 91 9 mixture of (Z)-3/( )-3 to be obtained on a 0.5 mol scale. The diastereomeric purity of this mixture may be enhanced to 95 5 by treatment with 0.15 equivalents of benzaldehyde, since ( )-l-mcthyl-2-butenylboronatc ( )-3 is more reactive than (Z)-3. Repetition of this process provides (Z)-3 that is 98% isomerically pure. 

Either diastereomer 2 or 3 may be preferentially produced with high selectivity depending on the nature of the enolate counterion present2642-44. Mechanistic details of the diastercofacial differentiation process are not clear in many cases the diastereomeric ratio of the products exhibits a complex dependence on stoichiometry, enolate counterion and reaction conditions26. The dependence of the d.r. on the nature of the enolate counterion is roughly outlined (vide supra) while examples of conditions employed for the reaction of the enolates 1 with prochiral aldehydes arc listed (Table 4). 

The method is very useful for the synthesis of physiologically interesting a-mcthylamino acids, e.g., methyl dopa from the 3,4-dimethoxybenzyl derivative. The excellent stereoselection achieved in the process, however, is caused by the preferential crystallization of one pure diastereomerfrom the equilibrium mixture formed in the reversible Strecker reaction. Thus, the pure diastcrcomers with benzyl substituents, dissolved in chloroform or acetonitrile, give equilibrium mixtures of both diastereomers in a ratio of about 7 347. This effect has also been found for other s-methylamino nitriles of quite different structure49. If the amino nitrile (R1 = Bn) is synthesized in acetonitrile solution, the diastereomers do not crystallize while immediate hydrolysis indicates a ratio of the diastereomeric amino nitriles (S)I(R) of 86 1447. 

The Ugi reaction has been successfully applied to the synthesis of oligopeptide derivatives, c.g.. in the construction of a pure tetra-L-valine derivative69. The 2-methylpropanaldimine 2 of (/7)-l-ferroccnyl-2-rnethylpropylarnine with /V-formyl-L-2-amino-3-methylbulanoic acid (3) as the carboxylic acid component and methyl A/-[(.S)-2-isocyano-3-mcthyl-l -nxo-buLyl -L-2-aiuino-3-inethylbutanoate (4) furnishes the diastereomeric valyl-valyl-valyl-valine derivatives in a ratio (S,S[R],S,S)i(S,R[R],S,S) of 91 9. The stereoselectivity of the process can be enhanced to 98.5 1.5 when two equivalents of tetraethylammonium A -formylvalinate are added. 

RCM of a dienyne was also a key step in Mori s recent total synthesis of the alkaloid erythrocarine (447) [183]. The tetracyclic framework of447 was elaborated in the penultimate step, by exposing the hydrochloride of metathesis precursor 445 (1 1 diastereomeric mixture at the carbinol center) to first-generation catalyst A. The tandem process occurred smoothly within 18 h at room temperature leading to tetracycles 446 (1 1 mixture) in quantitative yield. Deprotection of the a-acetoxy isomer 446a led to 447 (Scheme 88). 

A related situation is found in the case of P-substituted cycloketones here, the electronic difference between the two a-carbons is almost insignificant, resulting in unselective migration upon chemical oxidation. BVMOs have a particularly different behavior, as they can influence the stereo- and/or regioselectivity of the biooxidation. In the latter case, the distribution of proximal and distal lactones is affected by directing the oxygen insertion process either into the bond close or remote to the position of the P-substituent. Consequently, a regioisomeric excess (re) can be defined for this biotransformation, similar to enantiomeric excess or diastereomeric excess values [143]. 

The intermolecular Pauson-Khand reaction of the resulting S/P-cobalt complexes with norbornadiene was studied under thermal and A -oxide activation conditions. Thus, heating the diastereomerically pure complex (R = Ph, R = Cy) with ten equivalents of norbornadiene at 50 °C in toluene afforded the corresponding exo-cyclopentenone in a quantitative yield and with an enantio-selectivity of 99% ee. Under similar conditions, the analogous trimethylsilyl complex (R = TMS, R = Cy) afforded the expected product in a high yield but with a lower enantioselectivity of 57% ee. In order to increase this enantio-selectivity, these authors performed this reaction at room temperature in dichloromethane as the solvent and in the presence of NMO, which allowed an enantioselectivity of 97% ee to be reached. These authors assumed that the thermal activation promoted the isomerisation of the S/P ligand leading to a nonstereoselective process. 

The unique feature of the Horner-Wittig reaction is that the addition intermediate can be isolated and purified, which provides a means for control of the reaction s stereochemistry. It is possible to separate the two diastereomeric adducts in order to prepare the pure alkenes. The elimination process is syn, so the stereochemistry of the alkene that is formed depends on the stereochemistry of the adduct. Usually the anti adduct is the major product, so it is the Z-alkene that is favored. The syn adduct is most easily obtained by reduction of (3-ketophosphine oxides.269... 

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